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用于长期自发收缩心肌细胞培养的微流控制造三维细胞外基质支架

Three-dimensional extracellular matrix scaffolds by microfluidic fabrication for long-term spontaneously contracted cardiomyocyte culture.

作者信息

Mei Jeng-Chun, Wu Aden Yuan Kun, Wu Po-Chen, Cheng Nai-Chen, Tsai Wei-Bor, Yu Jiashing

机构信息

1 Department of Chemical Engineering, National Taiwan University , Taipei, Taiwan .

出版信息

Tissue Eng Part A. 2014 Nov;20(21-22):2931-41. doi: 10.1089/ten.TEA.2013.0549. Epub 2014 Jul 22.

DOI:10.1089/ten.TEA.2013.0549
PMID:24851797
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4229871/
Abstract

To repair damaged cardiac tissue, the important principle of in vitro cell culture is to mimic the in vivo cell growth environment. Thus, micro-sized cells are more suitably cultured in three-dimensional (3D) than in two-dimensional (2D) microenvironments (ex: culture dish). With the matching dimensions of works produced by microfluidic technology, chemical engineering and biochemistry applications have used this technology extensively in cellular works. The 3D scaffolds produced in our investigation has essential properties, such has high mass transfer efficiency, and variable pore sizes, to adapt to various needs of different cell types. In addition to the malleability of these innovative scaffolds, fabrication procedure was effortless and fast. Primary neonatal mice cardiomyocytes were successfully harvested and cultured in 3D scaffolds made of gelatin and collagen. Gelatin and gelatin-collagen scaffold were produced by the formation of microbubbles through a microfluidic device, and the mechanical properties of gelatin scaffold and gelatin-collagen scaffold were measured. Cellular properties in the microbubbles were also monitored. Fluorescence staining results assured that cardiomyocytes could maintain in vivo morphology in 3D gelatin scaffold. In addition, it was found that 3D scaffold could prolong the contraction behavior of cardiomyocytes compared with a conventional 2D culture dish. Spontaneously contracted behavior was maintained for the longest (about 1 month) in the 3D gelatin scaffold, about 19 days in the 3D gelatin-collagen scaffold. To sum up, this 3D platform for cell culture has promising potential for myocardial tissue engineering.

摘要

为了修复受损的心脏组织,体外细胞培养的重要原则是模拟体内细胞生长环境。因此,与二维(2D)微环境(如培养皿)相比,微小细胞更适合在三维(3D)环境中培养。由于微流控技术所产生的结构尺寸匹配,化学工程和生物化学应用已在细胞研究中广泛使用该技术。我们研究中制备的3D支架具有诸如高传质效率和可变孔径等基本特性,以适应不同细胞类型的各种需求。除了这些创新支架的可塑性外,制造过程轻松且快速。原代新生小鼠心肌细胞成功收获并培养在由明胶和胶原蛋白制成的3D支架中。通过微流控装置形成微泡来制备明胶和明胶 - 胶原蛋白支架,并测量明胶支架和明胶 - 胶原蛋白支架的力学性能。还监测了微泡中的细胞特性。荧光染色结果证实心肌细胞在3D明胶支架中可以保持体内形态。此外,发现与传统的2D培养皿相比,3D支架可以延长心肌细胞的收缩行为。在3D明胶支架中,自发收缩行为维持最长时间(约1个月),在3D明胶 - 胶原蛋白支架中约为19天。总之,这个用于细胞培养的3D平台在心肌组织工程方面具有广阔的潜力。

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